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婴幼儿胸腺细胞中HIV-1表达的体外研究。

In vitro studies of HIV-1 expression in thymocytes from infants and children.

作者信息

Hays E F, Uittenbogaart C H, Brewer J C, Vollger L W, Zack J A

机构信息

Department of Medicine, University of California, Los Angeles.

出版信息

AIDS. 1992 Mar;6(3):265-72. doi: 10.1097/00002030-199203000-00003.

Abstract

OBJECTIVE

To determine whether thymocytes from infants and young children can be infected with and their maturation capability altered by HIV-1, and to examine the effects of interleukin (IL)-2 and IL-4 on this process.

DESIGN

Serum-free culture medium was used so that cytokine effects could be studied under defined conditions. The primary virus isolates HIV-1JR-CSF and HIV-1JR-FL were used because their effects should most closely resemble those of viruses which might be found in an infected child.

METHODS

Thymocytes from infants and young children were infected with virus and cultured in serum-free medium with the cytokines IL-2 and IL-4 alone or in combination. HIV-1 expression was measured after 12 days by p24 levels in culture supernatants. Thymocyte maturation was determined by changes in surface phenotype, as measured by flow cytometry.

RESULTS

HIV-1 expression by thymocytes, which increased with time of culture, occurred when thymocytes were cultured with each cytokine. p24 levels were slightly increased when cultured with IL-2, compared with IL-4. Virus expression was remarkably increased when the cytokines were combined in culture. This expression was synergistic rather than additive. The synergy, evident in mature, but not immature thymocytes, was demonstrated with both pharmacologic and physiologic concentrations of cytokines. T-cells from peripheral blood cultured under the same conditions demonstrated lower virus expression in the presence of cytokines and synergy was not shown. Cytokine-induced thymocyte maturation and thymocyte survival in vitro was unimpaired by infection with HIV-1.

CONCLUSIONS

These findings indicate that the cytokines IL-2 and IL-4, which are normally present in the thymic environment, can synergize to promote HIV-1 expression by thymocytes infected in vitro. This occurs without impairing the maturation induced by these cytokines. Thus, the mature thymocyte may provide a continuous supply of virus-expressing T-cells to the peripheral blood and lymphoid tissues of the infected child.

摘要

目的

确定婴幼儿胸腺细胞是否可被HIV-1感染并使其成熟能力发生改变,并研究白细胞介素(IL)-2和IL-4在此过程中的作用。

设计

使用无血清培养基,以便在特定条件下研究细胞因子的作用。使用原发性病毒分离株HIV-1JR-CSF和HIV-1JR-FL,因为它们的作用应与感染儿童体内可能发现的病毒作用最为相似。

方法

用病毒感染婴幼儿胸腺细胞,并在无血清培养基中单独或联合使用细胞因子IL-2和IL-4进行培养。培养12天后,通过培养上清液中的p24水平测量HIV-1表达。通过流式细胞术测量表面表型的变化来确定胸腺细胞成熟度。

结果

当胸腺细胞与每种细胞因子一起培养时,胸腺细胞的HIV-1表达随培养时间增加。与IL-4相比,用IL-2培养时p24水平略有升高。当细胞因子在培养中联合使用时,病毒表达显著增加。这种表达是协同的而非相加的。在成熟而非未成熟的胸腺细胞中明显的协同作用,在细胞因子的药理和生理浓度下均得到证实。在相同条件下培养的外周血T细胞在存在细胞因子时显示出较低的病毒表达,且未显示协同作用。HIV-1感染并未损害细胞因子诱导的胸腺细胞成熟和体外胸腺细胞存活。

结论

这些发现表明,胸腺环境中通常存在的细胞因子IL-2和IL-4可协同促进体外感染的胸腺细胞表达HIV-1。这一过程不会损害这些细胞因子诱导的成熟。因此,成熟的胸腺细胞可能为受感染儿童的外周血和淋巴组织持续提供表达病毒的T细胞。

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